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Modular ssDNA binding and inhibition of telomerase activity by designer PPR proteins.

Nat Commun. 2018-06; 
SpåhrHenrik,ChiaTiongsun,LingfordJames P,SiiraStefan J,CohenScott B,FilipovskaAleksandra,RackhamOl
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Gene Synthesis … 1b for a detailed example). Synthetic genes encoding the final cPPR design were optimised for expression in Escherichia coli and synthesised from overlapping oligonucleotides (GeneArt and GenScript). Protein purification … Get A Quote

摘要

DNA is typically found as a double helix, however it must be separated into single strands during all phases of DNA metabolism; including transcription, replication, recombination and repair. Although recent breakthroughs have enabled the design of modular RNA- and double-stranded DNA-binding proteins, there are currently no tools available to manipulate single-stranded DNA (ssDNA). Here we show that artificial pentatricopeptide repeat (PPR) proteins can be programmed for sequence-specific ssDNA binding. Interactions occur using the same code and specificity as for RNA binding. We solve the structures of DNA-bound and apo proteins revealing the basis for ssDNA binding and how hydrogen bond rearrangement... More

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